Allele-specific aberration of imprinted domain chromosome architecture associates with large offspring syndrome

Yahan Li; Frimpong Boadu; Max R Highsmith; Darren E Hagen; Jianlin Cheng; Rocío Melissa Rivera

doi:10.1016/j.isci.2022.104269

Allele-specific aberration of imprinted domain chromosome architecture associates with large offspring syndrome

iScience. 2022 Apr 20;25(5):104269. doi: 10.1016/j.isci.2022.104269. eCollection 2022 May 20.

Authors

Yahan Li¹, Frimpong Boadu², Max R Highsmith², Darren E Hagen³, Jianlin Cheng², Rocío Melissa Rivera¹

Affiliations

¹ Division of Animal Sciences, University of Missouri, Columbia, MO 65211, USA.
² Department of Electrical Engineering and Computer Science, University of Missouri, Columbia, MO 65211, USA.
³ Department of Animal and Food Science, Oklahoma State University, Stillwater, OK 74078, USA.

Abstract

Large offspring syndrome (LOS) and Beckwith-Wiedemann syndrome are similar epigenetic congenital overgrowth conditions in ruminants and humans, respectively. We have reported global loss-of-imprinting, methylome epimutations, and gene misregulation in LOS. However, less than 4% of gene misregulation can be explained with short range (<20kb) alterations in DNA methylation. Therefore, we hypothesized that methylome epimutations in LOS affect chromosome architecture which results in misregulation of genes located at distances >20kb in cis and in trans (other chromosomes). Our analyses focused on two imprinted domains that frequently reveal misregulation in these syndromes, namely KvDMR1 and IGF2R. Using bovine fetal fibroblasts, we identified CTCF binding at IGF2R imprinting control region but not KvDMR1, and allele-specific chromosome architecture of these domains in controls. In LOS, analyses identified erroneous long-range contacts and clustering tendency in the direction of expression of misregulated genes. In conclusion, altered chromosome architecture is associated with LOS.

Keywords: Biological sciences; Genetics; molecular biology.